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在无剪切应力情况下VLA - 4/VCAM - 1相互作用的分子解离速率与细胞解离速率之间的关系。

Relationship between molecular and cellular dissociation rates for VLA-4/VCAM-1 interaction in the absence of shear stress.

作者信息

Zwartz Gordon, Chigaev Alexandre, Foutz Terry, Larson Richard S, Posner Richard, Sklar Larry A

机构信息

Department of Pathology and Cancer Center, University of New Mexico Health Sciences Center, Albuquerque, New Mexico 87131, USA.

出版信息

Biophys J. 2004 Feb;86(2):1243-52. doi: 10.1016/S0006-3495(04)74198-3.

Abstract

The rate of leukocyte recruitment to and detachment from the vasculature contributes to cellular tethering, rolling, firm adherence, and migration across an endothelium layer. The molecular rates depend on the type and number of bound integrin or selectin adhesion molecules, shear force acting on the bound adhesion molecules, and affinity state of integrins. Although little is known of the effect that the number of adhesion molecules has on leukocyte recruitment, it has been shown that firm adhesion for cells in suspension may be mediated by small numbers of bound adhesion molecules. We studied the disaggregation of aggregates composed of B78H1 cells transfected with human vascular cell adhesion molecule-1 (VCAM-1) and human monoblastoid U937 cells expressing Very Late Antigen-4 (VLA-4). Aggregate disaggregation rates were obtained and compared to dissociation rates for soluble rhVCAM-1 ligand and monoblastoid U937 cells. Under conditions without shear stress, it was found that average cellular disaggregation rates were a factor of 1.3 +/- 0.4 times slower than molecular dissociation rates for the 1 mM Mn(2+) and 1 mM Mn(2+) + 1 mM Ca(2+) conditions. A simple mathematical model was used to predict how much smaller the dissociation constant would be if the number of bonds holding an aggregate varied from one bond to N bonds under conditions without shear stress. The average number of adhesion bonds holding the cell aggregates together was found to be 1.5 +/- 0.7. This suggests that a few bonds were needed to form cellular aggregates and that increased aggregation was related to integrin affinity changes and not due to clustering or increased bond numbers.

摘要

白细胞募集到血管系统以及从血管系统脱离的速率,对细胞的系留、滚动、牢固黏附以及在内皮细胞层上的迁移都有影响。分子速率取决于结合的整合素或选择素黏附分子的类型和数量、作用于结合的黏附分子上的剪切力以及整合素的亲和力状态。尽管对于黏附分子数量对白细胞募集的影响了解甚少,但已表明悬浮细胞的牢固黏附可能由少量结合的黏附分子介导。我们研究了由转染了人血管细胞黏附分子-1(VCAM-1)的B78H1细胞和表达极迟抗原-4(VLA-4)的人单核细胞样U937细胞组成的聚集体的解聚情况。获得了聚集体解聚速率,并与可溶性重组人VCAM-1配体和单核细胞样U937细胞的解离速率进行了比较。在无剪切应力的条件下,发现在1 mM Mn(2+)和1 mM Mn(2+) + 1 mM Ca(2+)条件下,平均细胞解聚速率比分子解离速率慢1.3 +/- 0.4倍。使用一个简单的数学模型来预测在无剪切应力条件下,维持聚集体的键数从一个键变化到N个键时,解离常数会小多少。发现将细胞聚集体维系在一起的黏附键的平均数量为1.5 +/- 0.7。这表明形成细胞聚集体需要少数几个键,并且聚集体增加与整合素亲和力变化有关,而不是由于聚集或键数增加。

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